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Syntheses and biological evaluation of 2-amino-3-acyl-tetrahydrobenzothiophene derivatives; antibacterial agents with antivirulence activity

机译:2-氨基-3-酰基-四氢苯并噻吩衍生物的合成及生物学评价;具有抗毒活性的抗菌剂

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摘要

Developing new compounds targeting virulence factors (e.g., inhibition of pilus assembly by pilicides) is a promising approach to combating bacterial infection. A high-throughput screening campaign of a library of 17,500 small molecules identified 2-amino-3-acyl-tetrahydrobenzothiophene derivatives (hits >2 and >3) as novel inhibitors of pili-dependent biofilm formation in an uropathogenic Escherichia coli strain UTI89. Based on compounds >2 and >3 as a starting point, we designed and synthesized a series of structurally related analogs and investigated their activity against biofilm formation of E.coli UTI89. Systematic structural modification of the initial hits provided valuable information on their SARs for further optimization. In addition, small structural changes to the parent molecules resulted in low micromolar inhibitors (>20–23) of E.coli biofilm development without effect on bacterial growth. The hit compound >3 and its analog >20 were confirmed to prevent pili formation in a hemagglutination (HA) titer assay and electron microscopy (EM) measurements. These findings suggest that 2-amino-3-acyl-tetrahydrobenzothiophenes may serve as a new class of compounds for further elaboration as antibacterial agents with antivirulence activity.
机译:研发针对毒力因子的新化合物(例如,杀真菌剂抑制菌毛组装)是对抗细菌感染的有前途的方法。在一个由17,500个小分子组成的库中进行的高通量筛选活动中,确定了2-氨基-3-酰基-四氢苯并噻吩衍生物(命中> 2 和> 3 )为pili-新颖抑制剂尿毒症性大肠杆菌UTI89菌株中依赖的生物膜形成。基于化合物> 2 和> 3 作为出发点,我们设计并合成了一系列结构相关的类似物,并研究了它们对大肠杆菌UTI89生物膜形成的活性。初始命中的系统结构修改为它们的SAR提供了有价值的信息,可用于进一步优化。此外,对母体分子的微小结构变化导致大肠杆菌生物膜发育的低微摩尔抑制剂(> 20-23 )对细菌生长没有影响。在血凝(HA)滴度测定法和电子显微镜(EM)测量中,确定了命中化合物> 3 及其类似物> 20 可防止菌毛形成。这些发现表明2-氨基-3-酰基-四氢苯并噻吩可作为一类新的化合物,进一步用作具有抗毒活性的抗菌剂。

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